XB-ART-47025
J Biol Chem
2013 Jun 21;28825:18366-80. doi: 10.1074/jbc.M113.469882.
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The Lhs1/GRP170 chaperones facilitate the endoplasmic reticulum-associated degradation of the epithelial sodium channel.
Buck TM
,
Plavchak L
,
Roy A
,
Donnelly BF
,
Kashlan OB
,
Kleyman TR
,
Subramanya AR
,
Brodsky JL
.
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The epithelial sodium channel, ENaC, plays a critical role in maintaining salt and water homeostasis, and not surprisingly defects in ENaC function are associated with disease. Like many other membrane-spanning proteins, this trimeric protein complex folds and assembles inefficiently in the endoplasmic reticulum (ER), which results in a substantial percentage of the channel being targeted for ER-associated degradation (ERAD). Because the spectrum of factors that facilitates the degradation of ENaC is incomplete, we developed yeast expression systems for each ENaC subunit. We discovered that a conserved Hsp70-like chaperone, Lhs1, is required for maximal turnover of the ENaC α subunit. By expressing Lhs1 ATP binding mutants, we also found that the nucleotide exchange properties of this chaperone are dispensable for ENaC degradation. Consistent with the precipitation of an Lhs1-αENaC complex, Lhs1 holdase activity was instead most likely required to support the ERAD of αENaC. Moreover, a complex containing the mammalian Lhs1 homolog GRP170 and αENaC co-precipitated, and GRP170 also facilitated ENaC degradation in human, HEK293 cells, and in a Xenopus oocyte expression system. In both yeast and higher cell types, the effect of Lhs1 on the ERAD of αENaC was selective for the unglycosylated form of the protein. These data establish the first evidence that Lhs1/Grp170 chaperones can act as mediators of ERAD substrate selection.
???displayArticle.pubmedLink??? 23645669
???displayArticle.pmcLink??? PMC3689978
???displayArticle.link??? J Biol Chem
???displayArticle.grants??? [+]
P30 DK079307 NIDDK NIH HHS , R01 DK065161 NIDDK NIH HHS , DK65161 NIDDK NIH HHS , DK79307 NIDDK NIH HHS , GM75061 NIGMS NIH HHS , K01 DK090195 NIDDK NIH HHS , K01DK090195 NIDDK NIH HHS , P30 DK072506 NIDDK NIH HHS , R56 DK065161 NIDDK NIH HHS , R01 GM075061 NIGMS NIH HHS
Species referenced: Xenopus
Genes referenced: hsp70 hspa1l
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